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组蛋白缺陷的抑制子分析确定了hda1复合体在染色体分离中的新功能。

Suppressor analysis of a histone defect identifies a new function for the hda1 complex in chromosome segregation.

作者信息

Kanta Hasna, Laprade Lisa, Almutairi Abeer, Pinto Inés

机构信息

Department of Biological Sciences, University of Arkansas, Fayetteville 72701, USA.

出版信息

Genetics. 2006 May;173(1):435-50. doi: 10.1534/genetics.105.050559. Epub 2006 Jan 16.

Abstract

Histones are essential for the compaction of DNA into chromatin and therefore participate in all chromosomal functions. Specific mutations in HTA1, one of the two Saccharomyces cerevisiae genes encoding histone H2A, have been previously shown to cause chromosome segregation defects, including an increase in ploidy associated with altered pericentromeric chromatin structure, suggesting a role for histone H2A in kinetochore function. To identify proteins that may interact with histone H2A in the control of ploidy and chromosome segregation, we performed a genetic screen for suppressors of the increase-in-ploidy phenotype associated with one of the H2A mutations. We identified five genes, HHT1, MKS1, HDA1, HDA2, and HDA3, four of which encode proteins directly connected to chromatin function: histone H3 and each of the three subunits of the Hda1 histone deacetylase complex. Our results show that Hda3 has functions distinct from Hda2 and Hda1 and that it is required for normal chromosome segregation and cell cycle progression. In addition, HDA3 shows genetic interactions with kinetochore components, emphasizing a role in centromere function, and all three Hda proteins show association with centromeric DNA. These findings suggest that the Hda1 deacetylase complex affects histone function at the centromere and that Hda3 has a distinctive participation in chromosome segregation. Moreover, these suppressors provide the basis for future studies regarding histone function in chromosome segregation.

摘要

组蛋白对于将DNA压缩成染色质至关重要,因此参与所有染色体功能。酿酒酵母中编码组蛋白H2A的两个基因之一HTA1的特定突变,先前已被证明会导致染色体分离缺陷,包括与着丝粒周围染色质结构改变相关的倍性增加,这表明组蛋白H2A在动粒功能中发挥作用。为了鉴定在倍性和染色体分离控制中可能与组蛋白H2A相互作用的蛋白质,我们针对与一种H2A突变相关的倍性增加表型的抑制子进行了遗传筛选。我们鉴定出五个基因,即HHT1、MKS1、HDA1、HDA2和HDA3,其中四个基因编码与染色质功能直接相关的蛋白质:组蛋白H3以及Hda1组蛋白去乙酰化酶复合体的三个亚基中的每一个。我们的结果表明,Hda3具有与Hda2和Hda1不同的功能,并且它是正常染色体分离和细胞周期进程所必需的。此外,HDA3与动粒成分存在遗传相互作用,强调了其在着丝粒功能中的作用,并且所有三种Hda蛋白都显示与着丝粒DNA相关联。这些发现表明,Hda1去乙酰化酶复合体影响着丝粒处的组蛋白功能,并且Hda3在染色体分离中具有独特的作用。此外,这些抑制子为未来关于组蛋白在染色体分离中功能的研究提供了基础。

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